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Targeting the cytoskeleton to direct pancreatic differentiation of human pluripotent stem cells.
Citation | “Targeting The Cytoskeleton To Direct Pancreatic Differentiation Of Human Pluripotent Stem Cells.”. Nature Biotechnology, pp. 460-470. . |
Center | Washington University in St Louis |
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Author | Nathaniel J Hogrebe, Punn Augsornworawat, Kristina G Maxwell, Leonardo Velazco-Cruz, Jeffrey R Millman |
Abstract |
Generation of pancreatic β cells from human pluripotent stem cells (hPSCs) holds promise as a cell replacement therapy for diabetes. In this study, we establish a link between the state of the actin cytoskeleton and the expression of pancreatic transcription factors that drive pancreatic lineage specification. Bulk and single-cell RNA sequencing demonstrated that different degrees of actin polymerization biased cells toward various endodermal lineages and that conditions favoring a polymerized cytoskeleton strongly inhibited neurogenin 3-induced endocrine differentiation. Using latrunculin A to depolymerize the cytoskeleton during endocrine induction, we developed a two-dimensional differentiation protocol for generating human pluripotent stem-cell-derived β (SC-β) cells with improved in vitro and in vivo function. SC-β cells differentiated from four hPSC lines exhibited first- and second-phase dynamic glucose-stimulated insulin secretion. Transplantation of islet-sized aggregates of these cells rapidly reversed severe preexisting diabetes in mice at a rate close to that of human islets and maintained normoglycemia for at least 9 months. |
Year of Publication |
2020
|
Journal |
Nature biotechnology
|
Volume |
38
|
Issue |
4
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Number of Pages |
460-470
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Date Published |
04/2020
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ISSN Number |
1546-1696
|
DOI |
10.1038/s41587-020-0430-6
|
Alternate Journal |
Nat. Biotechnol.
|
PMID |
32094658
|
PMCID |
PMC7274216
|
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